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Serum surfactant protein D as a marker for bronchopulmonary dysplasia

机译:血清表面活性剂蛋白D作为支气管扩张发育不良的标志物

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Background: Lung epithelial cells express surfactant protein D (SP-D), a calcium-dependent lectin that plays an important role in antibody-independent pulmonary host defense. Previous studies have shown that it is found in the peripheral circulation in patients with pulmonary disease, likely because of translocation into the blood when lung epithelial barriers are disrupted by inflammation or acute injury. In adults, serum SP-D levels are biomarkers for the progression and severity of chronic lung disease. In neonates, elevated SP-D levels in cord blood and on day 1 have been associated with prenatal risk factors and with an increased risk of respiratory distress syndrome and infections. It is not known whether serum SP-D during the first week of life is a marker for bronchopulmonary dysplasia (BPD), a form of chronic lung disease of prematurity that is associated with lung parenchymal maldevelopment and injury. Objective: The goal of this study is to determine whether serum SP-D on days 3 and 7 of life are associated with the development of BPD in preterm infants. Design/methods: Serum samples were obtained on postnatal days 3 and 7 from 106 preterm infants (500-2000 g birth weight, 23-32-week gestation). SP-D was quantified by Western blot. BPD was determined at 36 weeks PMA using NICHD criteria. Results: The mean birth weight was 1145 +/- 347 g and gestational age 29.2 +/- 7.4 weeks. BPD was diagnosed in 7 and "BPD or death" in 16 infants. Days 3 and 7 values tracked significantly (r = 0.648), and did not correlate with birth weight or gestational age. Contrary to expectations, serum SP-D was not associated with BPD. Significant gender differences were noted, with SP-D dropping from day 3 to day 7 in males, while increasing in females (p .05). Conclusion: Elevated serum SP-D does not appear to be a useful marker for BPD. Decreasing serum SP-D levels in males, as compared to females, during the first week of life are likely related to gender differences in lung maturation, consistent with the higher incidence of BPD in males.
机译:背景:肺上皮细胞表达表面活性剂蛋白D(SP-D),依赖于依赖于抗体无关的肺机宿主防御的重要作用。以前的研究表明,当肺上皮屏障被炎症或急性损伤中断时,它在肺病患者的外周循环中发现,可能是因为肿瘤上皮屏障被破坏或急性损伤时。在成人中,血清SP-D水平是慢性肺病的进展和严重程度的生物标志物。在新生儿中,脐带血的升高水平和第1天的水平与产前危险因素有关,并且呼吸窘迫综合征和感染的风险增加。尚不清楚血清SP-D是否在生命的第一周期间是支气管扩张发育不良(BPD)的标志物,其一种与肺部实质畸形和损伤有关的早熟的慢性肺病的形式。目的:本研究的目的是确定生命中第3天和第7天的血清SP-D是否与早产儿的BPD的发展有关。设计/方法:从106天的后期3和7中获得血清样品(500-2000g出生体重,23-32周妊娠)。 SP-D通过Western印迹量化。使用NichD标准在36周PMA测定BPD。结果:平均出生体重为1145 +/- 347克和孕龄29.2 +/- 7.4周。 BPD在16名婴儿中被诊断为7和“BPD或死亡”。第3天和7个值显着跟踪(r = 0.648),与出生体重或妊娠期没有相关。与期望相反,血清SP-D与BPD无关。注意到了重大的性别差异,SP-D从男性的第3天到第7天的SP-D滴,同时雌性增加(P <.05)。结论:血清SP-D升高似乎是BPD的有用标志物。与雌性相比,在雌性中减少血清SP-D水平,在第一周的生命中可能与肺成熟的性别差异有关,与男性BPD的发病率较高。

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